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Mouse development with a single E2F activator

机译:使用单个E2F激活剂进行鼠标开发

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The E2F family is conserved from Caenorhabditis elegans to mammals, with some family members having transcription activation functions and others having repressor functions. Whereas C. elegans and Drosophila melanogaster have a single E2F activator protein and repressor protein, mammals have at least three activator and five repressor proteins. Why such genetic complexity evolved in mammals is not known. To begin to evaluate this genetic complexity, we targeted the inactivation of the entire subset of activators, E2fl, E2f2, E2f3a and E2f3b, singly or in combination in mice. We demonstrate that E2f3a is sufficient to support mouse embryonic and postnatal development. Remarkably, expression of E2f3b or E2f1 from the E2f3a locus (E2f3a~(3bki) or E2f3a~(1ki), respectively) suppressed all the postnatal phenotypes associated with the inactivation of E2f3a. We conclude that there is significant functional redundancy among activators and that the specific requirement for E2f3a during postnatal development is dictated by regulatory sequences governing its selective spatiotemporal expression and not by its intrinsic protein functions. These findings provide a molecular basis for the observed specificity among E2F activators during development.
机译:E2F家族从秀丽隐杆线虫保存到哺乳动物,其中一些家族成员具有转录激活功能,而其他家族成员具有阻遏功能。秀丽隐杆线虫和果蝇仅具有一个E2F激活蛋白和阻遏蛋白,而哺乳动物则至少具有三个激活蛋白和五个阻遏蛋白。为何在哺乳动物中进化出如此复杂的遗传基因尚不清楚。为了开始评估这种遗传复杂性,我们针对小鼠中单独或组合的激活子E2f1,E2f2,E2f3a和E2f3b的整个子集进行了灭活。我们证明,E2f3a足以支持小鼠的胚胎和出生后的发展。值得注意的是,从E2f3a基因座(分别为E2f3a〜(3bki)或E2f3a〜(1ki))表达E2f3b或E2f1抑制了所有与E2f3a失活相关的产后表型。我们得出的结论是,激活剂之间存在显着的功能冗余,并且在产后发育过程中对E2f3a的特殊要求由控制其选择性时空表达的调控序列而非其固有的蛋白质功能决定。这些发现为开发过程中E2F激活剂之间观察到的特异性提供了分子基础。

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